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R 环衍生的细胞质 RNA-DNA 杂交体激活免疫反应。

R-loop-derived cytoplasmic RNA-DNA hybrids activate an immune response.

机构信息

Department of Chemical and Systems Biology, Stanford University, Stanford, CA, USA.

Biometrology Group, Division of Chemical and Biological Metrology, Korea Research Institute of Standards and Science, Daejeon, South Korea.

出版信息

Nature. 2023 Jan;613(7942):187-194. doi: 10.1038/s41586-022-05545-9. Epub 2022 Dec 21.

Abstract

R-loops are RNA-DNA-hybrid-containing nucleic acids with important cellular roles. Deregulation of R-loop dynamics can lead to DNA damage and genome instability, which has been linked to the action of endonucleases such as XPG. However, the mechanisms and cellular consequences of such processing have remained unclear. Here we identify a new population of RNA-DNA hybrids in the cytoplasm that are R-loop-processing products. When nuclear R-loops were perturbed by depleting the RNA-DNA helicase senataxin (SETX) or the breast cancer gene BRCA1 (refs. ), we observed XPG- and XPF-dependent cytoplasmic hybrid formation. We identify their source as a subset of stable, overlapping nuclear hybrids with a specific nucleotide signature. Cytoplasmic hybrids bind to the pattern recognition receptors cGAS and TLR3 (ref. ), activating IRF3 and inducing apoptosis. Excised hybrids and an R-loop-induced innate immune response were also observed in SETX-mutated cells from patients with ataxia oculomotor apraxia type 2 (ref. ) and in BRCA1-mutated cancer cells. These findings establish RNA-DNA hybrids as immunogenic species that aberrantly accumulate in the cytoplasm after R-loop processing, linking R-loop accumulation to cell death through the innate immune response. Aberrant R-loop processing and subsequent innate immune activation may contribute to many diseases, such as neurodegeneration and cancer.

摘要

R 环是含有 RNA-DNA 杂交的核酸,具有重要的细胞功能。R 环动力学的失调可导致 DNA 损伤和基因组不稳定性,这与内切酶如 XPG 的作用有关。然而,这种加工的机制和细胞后果仍不清楚。在这里,我们在细胞质中鉴定出一种新的 RNA-DNA 杂交体,它是 R 环加工产物。当核 R 环通过耗尽 RNA-DNA 解旋酶 senataxin(SETX)或乳腺癌基因 BRCA1(REFS.)来扰动时,我们观察到 XPG 和 XPF 依赖的细胞质杂交体的形成。我们确定其来源是一组具有特定核苷酸特征的稳定重叠核杂交体。细胞质杂交体与模式识别受体 cGAS 和 TLR3(REF)结合,激活 IRF3 并诱导细胞凋亡。从共济失调性眼球运动不能症 2 型(REF)患者的 SETX 突变细胞和 BRCA1 突变癌细胞中也观察到切除的杂交体和 R 环诱导的先天免疫反应。这些发现确立了 RNA-DNA 杂交体作为免疫原性物质,它们在 R 环加工后异常积累在细胞质中,通过先天免疫反应将 R 环积累与细胞死亡联系起来。异常的 R 环加工和随后的先天免疫激活可能导致许多疾病,如神经退行性疾病和癌症。

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